外阴硬化型地衣的免疫发病机制和免疫治疗:一项前瞻性队列研究

E. V. Kolesnikova, A. V. Zharov, M. A. Penzhoyan, D. I. Dupleeva
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After a clinical examination using the scale for assessing subjective and objective clinical signs of vulvar lichen sclerosus, 154 patients with a sclerosing variant of the disease course were selected for the study. The control cohort consisted of 30 women of the same age category without vulvar lichen sclerosus, taking into account the exclusion criteria. The study involved a clinical assessment (in points) of objective and subjective criteria characteristic of this variant of vulvar lichen sclerosus, as well as an assessment of the level of cytokines (interleukin-20; interleukin-23; interleukin-10; tumor necrosis factor α, interferon γ) in peripheral blood of the patients from the main and control groups. 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引用次数: 0

摘要

背景。目前,外阴硬化地衣的临床分类尚未统一登记(尚待登记?)分离其病程的病理和临床不同变异,使开发新的治疗方法成为可能。目标。结合外阴硬化性地衣的临床和免疫学特点,研究外阴硬化性地衣的发病机制。方法。2018 - 2022年在俄罗斯Krasonodar第二地区临床医院进行前瞻性队列研究,组织学诊断为外阴硬化苔藓292例,年龄20 ~ 70岁。采用外阴硬化地衣主客观临床体征评定量表进行临床检查后,选择154例具有硬化变异型病程的患者进行研究。参照排除标准,对照组包括30名无外阴地衣硬化的同龄女性。该研究包括对这种外阴硬化苔藓变异的客观和主观标准特征的临床评估(分),以及细胞因子水平的评估(白细胞介素-20;interleukin-23;白细胞介素- 10”;对照组与对照组患者外周血肿瘤坏死因子α、干扰素γ含量的变化。在用脱氧核糖核酸钠进行免疫治疗一个月后,作者评估其临床疗效(使用外阴痛数值评定量表和外阴瘙痒严重程度量表)和免疫学疗效(反复评估所研究细胞因子水平)。使用GraphPad Prism 6.0版本(GraphPad Software, Inc., San Diego, CA)对获得的数据进行分析和统计处理。结果。与外阴萎缩相比,外阴硬化症背景下的外阴皮肤色素沉着和增厚表现为外阴硬化症变异体。阴道前庭狭窄要么不存在(51.3%),要么主要对应于I级,其特异性低于色素沉着,甚至皮肤萎缩。主观体征包括严重外阴瘙痒,无或伴中度外阴痛(68.1%)。一项免疫学研究显示,白细胞介素-20水平有统计学意义的升高(p <0.0001),白细胞介素-23 (p <0.0001),干扰素γ (p <0.03),肿瘤坏死因子α (p <0.009),且抗炎白细胞介素-10水平显著降低(p <0.01)。与基线相比,白细胞介素-20 (p <0.0001),干扰素-γ和肿瘤坏死因子α (p <0.002),白细胞介素-23 (p <0.012),与对照组差异无统计学意义(除白细胞介素-23外,治疗后白细胞介素-23水平下降,但仍有统计学意义(p <0.01)。免疫治疗的临床疗效有统计学意义(p <0.001)治疗后外阴痛和外阴瘙痒减少。结论。所获得的数据表明,外阴硬化型地衣患者的临床特征和免疫学差异与正常女性相关,因此证明在该变体中使用脱氧核糖核酸钠具有临床和免疫学疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immune pathogenesis and immune therapy of a sclerosing variant of vulvar lichen sclerosus: a prospective cohort study
Background. Today, no unified clinical classification of vulvar lichen sclerosus is registered (is yet to be registered?). Isolation of pathogenetically and clinically different variants of its course enable new approaches to the treatment to be developed. Objective. To develop a pathogenetic therapy for the sclerosing variant of vulvar lichen sclerosus, taking into account its clinical and immunological characteristics. Methods. A prospective cohort study was conducted from 2018 to 2022 on the basis of Regional Clinical Hospital No. 2, Krasonodar, Russia. 292 patients aged 20 to 70 years were histologically diagnosed with vulvar lichen sclerosus. After a clinical examination using the scale for assessing subjective and objective clinical signs of vulvar lichen sclerosus, 154 patients with a sclerosing variant of the disease course were selected for the study. The control cohort consisted of 30 women of the same age category without vulvar lichen sclerosus, taking into account the exclusion criteria. The study involved a clinical assessment (in points) of objective and subjective criteria characteristic of this variant of vulvar lichen sclerosus, as well as an assessment of the level of cytokines (interleukin-20; interleukin-23; interleukin-10; tumor necrosis factor α, interferon γ) in peripheral blood of the patients from the main and control groups. One month after the immunotherapy with sodium deoxyribonucleate, the authors evaluated its clinical efficacy (using Numerical rating scale for pain (vulvodynia) and Vulvar pruritus severity scale) and immunological efficacy (repeated assessment of the level of the studied cytokines). Analysis and statistical processing of the obtained data were performed using Graph Pad Prism version 6.0 (GraphPad Software, Inc., San Diego, CA). Results . Depigmentation of the vulvar skin against the background of vulvar sclerosis and thickening features a sclerosing variant of vulvar lichen sclerosus compared to vulvar atrophy. Stenosis of the vaginal vestibule is either absent (51.3%) or predominantly corresponds to grade I, and is less specific than depigmentation and even skin atrophy. The subjective signs include a severe vulvar pruritus without or with moderately expressed (in 68.1%) vulvodynia. An immunological study showed a statistically significant increase in the level of interleukin-20 (p < 0.0001), interleukin-23 (p < 0.0001), interferon-γ (p < 0.03), tumor necrosis factor α (p < 0.009) in patients with maximal tissue sclerosis with respect to the control group, along with a statistically significant decrease in the level of anti-inflammatory interleukin-10 (p < 0.01). The immunological efficacy of sodium deoxyribonucleate was confirmed by a statistically significant (compared to baseline) decrease in interleukin-20 (p < 0.0001), interferon-γ and tumor necrosis factor α (p < 0.002), interleukin-23 (p < 0.012) without statistical differences with the control group (except for interleukin-23, the level of which decreased after therapy but remained statistically higher (p < 0.01) than in the control group). Clinical efficacy of immunotherapy was confirmed by a statistically significant (p < 0.001) reduction in vulvodynia and vulvar pruritus after the treatment. Conclusion . The obtained data demonstrate characteristic clinical features and immunological differences in relation to the norm in women with the sclerosing variant of vulvar lichen sclerosus, thereby justifying the use of sodium deoxyribonucleate in this variant with confirmed clinical and immunological efficacy.
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